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ERK pathway agonism for cancer therapy: evidence, insights, and a target discovery framework

Oleg Timofeev, Philippe Giron, Steffen Lawo, Martin Pichler, Amir Noeparast

2024npj Precision Oncology46 citationsDOIOpen Access PDF

Abstract

At least 40% of human cancers are associated with aberrant ERK pathway activity (ERKp). Inhibitors targeting various effectors within the ERKp have been developed and explored for over two decades. Conversely, a substantial body of evidence suggests that both normal human cells and, notably to a greater extent, cancer cells exhibit susceptibility to hyperactivation of ERKp. However, this vulnerability of cancer cells remains relatively unexplored. In this review, we reexamine the evidence on the selective lethality of highly elevated ERKp activity in human cancer cells of varying backgrounds. We synthesize the insights proposed for harnessing this vulnerability of ERK-associated cancers for therapeutical approaches and contextualize these insights within established pharmacological cancer-targeting models. Moreover, we compile the intriguing preclinical findings of ERK pathway agonism in diverse cancer models. Lastly, we present a conceptual framework for target discovery regarding ERKp agonism, emphasizing the utilization of mutual exclusivity among oncogenes to develop novel targeted therapies for precision oncology.

Topics & Concepts

MAPK/ERK pathwayAgonismCancerEffectorCancer cellBiologyCancer researchComputational biologyVulnerability (computing)NeuroscienceBioinformaticsMedicineSignal transductionImmunologyCell biologyGeneticsComputer sciencePolitical scienceLawComputer securityPoliticsMelanoma and MAPK PathwaysComputational Drug Discovery MethodsProtein Kinase Regulation and GTPase Signaling
ERK pathway agonism for cancer therapy: evidence, insights, and a target discovery framework | Litcius